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首页> 外文期刊>Journal of Virology >A new acute transforming feline retrovirus with fms homology specifies a C-terminally truncated version of the c-fms protein that is different from SM-feline sarcoma virus v-fms protein.
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A new acute transforming feline retrovirus with fms homology specifies a C-terminally truncated version of the c-fms protein that is different from SM-feline sarcoma virus v-fms protein.

机译:具有FMS同源性的新急性转化猫逆转录病毒指定了与SM-FINCE SARCOMA病毒V-FMS蛋白不同的C-Termiphly截断版本。

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摘要

The HZ5-feline sarcoma virus (FeSV) is a new acute transforming feline retrovirus which was isolated from a multicentric fibrosarcoma of a domestic cat. The HZ5-FeSV transforms fibroblasts in vitro and is replication defective. A biologically active integrated HZ5-FeSV provirus was molecularly cloned from cellular DNA of HZ5-FeSV-infected FRE-3A rat cells. The HZ5-FeSV has oncogene homology with the fms sequences of the SM-FeSV. The genome organization of the 8.6-kilobase HZ5-FeSV provirus is 5' delta gag-fms-delta pol-delta env 3'. The HZ5-and SM-FeSVs display indistinguishable in vitro transformation characteristics, and the structures of the gag-fms transforming genes in the two viruses are very similar. In the HZ5-FeSV and the SM-FeSV, identical c-fms and feline leukemia virus p10 sequences form the 5' gag-fms junction. With regard to v-fms the two viruses are homologous up to 11 amino acids before the C terminus of the SM-FeSV v-fms protein. In HZ5-FeSV a segment of 362 nucleotides then follows before the 3' recombination site with feline leukemia virus pol. The new 3' v-fms sequence encodes 27 amino acids before reaching a TGA termination signal. The relationship of this sequence with the recently characterized human c-fms sequence has been examined. The 3' HZ5-FeSV v-fms sequence is homologous with 3' c-fms sequences. A frameshift mutation (11-base-pair deletion) was found in the C-terminal fms coding sequence of the HZ5-FeSV. As a result, the HZ5-FeSV v-fms protein is predicted to be a C-terminally truncated version of c-fms. This frameshift mutation may determine the oncogenic properties of v-fms in the HZ5-FeSV.
机译:HZ5-猫科动物病毒(FESV)是一种新的急性转化猫科动物逆转录病毒,其来自国内猫的多中心纤维肉瘤。 Hz5-Fesv在体外转化成纤维细胞,并复制缺陷。从HZ5-Fesv感染的FES-3a大鼠细胞的细胞DNA分子克隆了生物活性的集成Hz5-Fesv潜水病。 HZ5-FESV对SM-Fesv的FMS序列具有癌基因同源性。 8.6千碱基Hz5-Fesv Provirus的基因组组织是5'Delta Gag-FMS-Delta pol-delta env 3'。 HZ5和SM-Fesvs在体外转化特性中脱节,并且两种病毒中的GAG-FMS转化基因的结构非常相似。在HZ5-FESV和SM-FESV,相同的C-FMS和猫型白血病病毒P10序列形成5'GAG-FMS结。关于V-FMS,两种病毒在SM-FESV V-FMS蛋白的C末端之前至多11个氨基酸。在Hz5-Fesv中,362个核苷酸的一段,然后在3'重组位点之前用猫患者白血病病毒Pol。在达到TGA终止信号之前,新的3'V-FMS序列编码27个氨基酸。已经研究了该序列与最近表征的人C-FMS序列的关系。 3'Hz5-Fesv V-FMS序列与3'C-FMS序列同源。在HZ5-FESV的C末端FMS编码序列中发现了框架突变(11-碱基对缺失)。结果,预测HZ5-Fesv V-FMS蛋白是C-inally截断的C-FMS。该帧突变突变可以确定HZ5-FESV中V-FMS的致癌性质。

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